Synthesis and Characterization of Novel Bifunctional Hemithioindigo

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ORGANIC LETTERS

Synthesis and Characterization of Novel Bifunctional Hemithioindigo Chromophores

2003 Vol. 5, No. 2 141-144

Wencke Steinle and Karola Ru1 ck-Braun* Technische UniVersita¨ t Berlin, Institut fu¨ r Chemie, Strasse des 17. Juni 135, D-10623 Berlin, Germany [email protected] Received October 14, 2002

ABSTRACT

General methods for the synthesis of novel bifunctional hemithioindigo (HT) compounds, e.g., ω-amino acid derivatives, are presented. The photochromic properties of the photoswitches have been characterized by UV−vis and 1H NMR spectroscopy.

Photochromic compounds are becoming increasingly popular for a series of biological applications based on the reversible photocontrol of the structure and function of biomolecules.1 Several approaches to photomodulating biological functions such as biocatalysis,2,3 ion transport,4,5 cell adhesion,6 protein folding,7 or membrane properties8 have been employed. Most of these studies involved the chemical modification of nucleotides, peptides, proteins, and lipids using azobenzenes (1) Willner, I.; Rubin, I. Angew. Chem., Int. Ed. Engl. 1996, 35, 367385. (2) (a) Yamazawa, A.; Liang, X.; Asanuma, H.; Komiyama, M. Angew. Chem., Int. Ed. 2000, 39, 2356-2357. (b) Asanuma, H.; Liang, X.; Yoshida, T.; Yamazawa, A.; Komiyama, M. Angew. Chem., Int. Ed. 2000, 39, 13161318. (3) James, D. A.; Burns, D. C.; Woolley, G. A. Protein Eng. 2001, 14, 983-991. (4) Osman, P.; Martin, S.; Milojevic, D.; Tansey, C.; Separovic, F. Langmuir 1998, 14, 4238-4242. (5) (a) Borisenko, V.; Burns, D. C.; Zhang, Z.; Woolley, G. A. J. Am. Chem. Soc. 2000, 122, 6364-6370. (b) Lien, L.; Dominic, C. J. J.; Zhang, Z.; Wooley, G. A. J. Am. Chem. Soc. 1996, 118, 12222-12223. (6) Haiqian, Z.; Hiroaki, S.; Ning, G.; Hiroshi, S.; Masahiko, S. J. Southeast UniV. 2001, 17, 22-26. (7) (a) Cattani-Scholz, A.; Renner, C.; Cabrele, C.; Behrendt, R.; Oesterhelt, D.; Moroder, L. Angew. Chem., Int. Ed. 2002, 41, 289-292. (b) Behrendt, R.; Renner, C.; Schenk, M.; Wang, F.; Wachtveitl, J.; Oesterhelt, D.; Moroder, L. Angew. Chem., Int. Ed. 1999, 38, 2771-2774. (c) Renner, C.; Cramer, J.; Behrendt, R.; Moroder, L. Biopolymers 2000, 54, 501-514. (d) Renner, C.; Behrendt, R.; Spo¨rlein, S.; Wachtveitl, J.; Moroder, L. Biopolymers 2000, 54, 489-500. (e) Renner, C.; Behrendt, 10.1021/ol027102+ CCC: $25.00 Published on Web 12/18/2002

© 2003 American Chemical Society

as reversible photoswitchable chromophores.2-7 In the past, one major strategy for proteins was random-chemical substitution of the chromophore to multiple undefined sites of the biomolecule.1 Nowadays, rational concepts focus on site-specific incorporation based on the design to photooperate not only steric or ion-dipole interactions but also conformational transitions of structural elements of proteins and peptides as, for example, β-turns and helices.7,9,10 In this context, novel chromophores with useful optical properties are gaining attention for tailor-made designs. Photochromic hemithioindigos are considered to be an interesting class of chromophore because of the frequent reversibility of the light-induced isomerizations or the thermal stability of the photochromic states among other beneficial properties.8,11-13 For example, Fyles reported on novel photoswitchable lipids R.; Heim, N.; Moroder, L. Biopolymers 2002, 63, 382-393. (f) Spo¨rlein, S.; Carstens, H.; Satzger, H.; Renner, C.; Behrendt, R.; Moroder, L.; Tavan, P.; Zinth, W.; Wachtveitl, J. PNAS 2002, 99, 7998-8002. (g) Behrendt, R.; Schenk, M.; Musiol, H.-J.; Moroder, L. J. Peptide Sci. 1999, 5, 519529. (8) Eggers, K.; Fyles, T. M.; Montoya-Pelaez, P. J. J. Org. Chem. 2001, 66, 2966-2977. (9) Ulysee, L.; Cubillos, J.; Chmielewski, J. J. Am. Chem. Soc. 1995, 117, 8466-8467. (10) (a) Kumita, J. R.; Smart, O. S.; Woolley, G. A. PNAS 2000, 97, 3803-3808. (b) Flint, D. G.; Kumita, J. R.; Smart, O. S.; Woolley, G. A. Chem. Biol. 2002, 9, 391-397.

containing a hemithioindigo chromophore as part of the fatty acid for the reversible control of membrane processes.8 Other hemithioindigo derivatives suitable for incorporation into biomolecules have, to our knowledge, never been explored. In this report we describe our approach to novel bifunctional hemithioindigo chromophores such as dicarboxylic acid esters and ω-amino acid-derivatives for incorporation into peptides and proteins. We initiated our studies starting from the literature-known thioindoxyl carboxylic acid chloride14 1 (Table 1) by examining the use of MeOH and

rable mixture of 3c and 3a in 64% yield in a ratio of 37:63 as determined by 1H NMR. Formation of 3a can be explained by tert-butyl ester cleavage and transesterification in the presence of hydrogen chloride during esterification of the carboxylic acid chloride. With triethylamine as an additive instead of pyridine, decomposition of thioindoxyl 1 took place in the presence of aldehyde 2c and methanol. Increasing the amount of piperidine (2.3 equiv) in the absence of pyridine afforded amide 4 (Scheme 1) in 54% yield (recrystallized from MeOH).

Scheme 1

Table 1. Synthesis of Hemithioindigo-Based Dicarboxylic Acid Esters 3

entry

aldehyde

3

R1

yielda (%)

1b

2a 2b 2c

3a 3b 3c

OCH2CO2Me CO2Me OCH2CO2tBu

50 50 52

2b 3b,c

a Isolated yields. b All reactions were carried out with 0.05-0.15 mL of piperidine as a catalyst. c Reaction was performed in the presence of 1.1 equiv of pyridine as an additive.

benzaldehydes 2a-c for the construction of compounds 3a,b as well as the selectively protected dicarboxylic acid ester 3c via simultaneous esterification in the 7-position and basecatalyzed aldol condensation in the 2-position. Various reaction conditions were examined, and a brief summary of the results obtained is presented in Table 1. The reactions of the thioindoxyl 1 with benzaldehydes 2a-c in the presence of methanol were generally carried out with piperidine as a catalyst.11 Hemithioindigos 3a and 3b were isolated in 50% yield after crystallization from 1:1 toluene/MeOH as yellow and orange powders, respectively, free from impurities and decomposition products. Chromatography on silica gel led to decomposition. By far, the cleanest reaction yielding 3c was obtained in the presence of 1.1 equiv of pyridine (52%, recrystallized from ether/pentane). Otherwise, the formation of substantial amounts of byproduct 3a was found, furnishing an insepa(11) (a) Yamaguchi, T.; Seki, T.; Tamaki, T.; Ichimura, K. Bull. Chem. Soc. Jpn. 1992, 65, 649-656. (b) Seki, T.; Tamaki, T.; Yamaguchi, T.; Ichimura, K. Bull. Chem. Soc. Jpn. 1992, 65, 657-663. (c) Ichimura, K.; Seki, T.; Tamaki, T.; Yamaguchi, T. Chem. Lett. 1990, 1645-1646. (12) Rea´monn, L. S. S.; O’Sullivan, W. I. J. Chem. Soc., Perkin Trans. 1 1977, 1009-1012. (13) (a) Mostoskavskii, M. A.; Izmail’skii, V. A. J. Gen. Chem. USSR 1961, 17, 21-31. (b) Mostoskavskii, M. A.; Izmail’skii, V. A. J. Gen. Chem. USSR 1963, 33, 727-731. (c) Mostoskavskii, M. A.; Izmail’skii, V. A. J. Gen. Chem. USSR 1965, 35, 519-523. (14) Irie, M.; Kato, M. J. Am. Chem. Soc. 1985, 107, 1024-1028. 142

We then prepared hemithioindigo ω-amino acid derivative 6 starting from 1, aldehyde 5, and methanol by applying exactly the same conditions as for 3c. But surprisingly the reactions produced inconsistent results regarding yield and purity (entry 1, Table 2). Thus, the reaction conditions were

Table 2. Synthesis of the ω-Amino Acid Derivative 6

MeOH 1 5 pyridine conversion of 5 yield entry (equiv) (equiv) (equiv) (equiv) (%) (%)a 1 2 3

5 5 7.5

1.0 1.0b 1.5b

1.1 1.0 1.0

1.1 13 19.5

61 81 98

79 98 98

a Yield of isolated crude material 6. b Reaction was carried out in the presence of 4 Å MS.

optimized with a sequential reaction protocol of esterification of thioindoxyl carboxylic acid chloride 1 prior to the Org. Lett., Vol. 5, No. 2, 2003

piperidine-catalyzed aldol condensation in degassed solution. Turnover and yield of ω-amino acid derivative 6 were improved up to 98% by increasing the number of equivalents of MeOH and pyridine (entries 2 and 3, Table 2) in the presence of 4 Å molecular sieves. The material contained only tiny amounts of byproduct, presumably due to the oxidation of excess thioindoxyl precursor and esterification intermediate. However, deprotection strategies were investigated with the functionalized hemithioindigos 3a-c and 4 before further optimizations of the reaction protocols. Deprotection of hemithioindigo tert-butyl esters with 1:1 TFA/DCM and 90:2:2 TFA/TIPS/H2O produced no isolable compounds.15,16 The decomposition is explained as a consequence of carbocation attack on sulfur and/or hydride attack on the R,β-unsaturated carbonyl moiety. Alternatively, reactions employing reagent K (TFA/water/thioanisole/phenol/ ethanedithiole) at room temperature were very promising and gave, for example, compound 7 in 80% yield (Scheme 1). However, for deprotection of the N-Boc-protected hemithioindigo compound 6, treatment with HCl in dioxane proved to be superior, yielding the salt 8 quantitatively. All attempts to selectively deprotect hemithioindigo methyl esters proved to be a challenge. Experiments under basic conditions (LiOH/THF, KOtBu/Et2O/H2O, NaOH/MeOH, Ba(OH)2/MeOH, NaOH/DMF/H2O) failed.15,16 Decomposition of the hemithioindigo core unit was observed, presumably via retro-aldol reaction because of the presence of the aldehyde precursors determined by 1H NMR spectroscopy of the crude reaction products. Similarly, exposure of 3a to Me3SiCl/NaI in MeCN or NaCN/LiI in DMF at elevated temperatures led to decomposition.15-17 Fortunately, the application of PhSH and K2CO3 in NMP at 190 °C gave product 9 in 89% yield (Scheme 2).18

Scheme 2

However, this deprotection procedure requires careful purification of the starting material. Therefore, the direct synthesis of N-Boc-protected ω-amino acid 10 was investigated next (Scheme 3). In a final series of experiments, reaction of 1 (1.5 equiv) with benzaldehyde 5 (1 equiv) in 7:3 NaOH(1%)/tBuOH performed very well. Heating at reflux led to complete consumption of the aldehyde within (15) Kocienski, P. J. Protecting Groups; Georg Thieme Verlag: Stuttgart, 1994. (16) Green, T. W.; Wuts, P. G. M. ProtectiVe Groups in Organic Synthesis; Wiley & Sons: New York, 1999. (17) Olah, G. A.; Husain, A.; Singh, B. P.; Mehrotra, A. K. J. Org. Chem. 1983, 48, 3667-3671. (18) Sharma, L.; Nayak, M. K.; Chakraborti, A. K. Tetrahedron 1999, 55, 9595-9600. Org. Lett., Vol. 5, No. 2, 2003

Scheme 3

3 h. Compound 10 was purified by chromatography on Florisil and isolated in 80% yield. First attempts to apply N-Boc-protected ω-amino acid 10 in peptide synthesis proved to be successful. Treatment of 10 with (S)-H-Lys(Cbz)-OMexHCl in the presence of HOBt, EDC, and DIEA in DMF furnished dipeptide 11 in 88% isolated yield (Scheme 4).7g

Scheme 4

After demonstrating the feasibility of the synthesis of bifunctional hemithioindigo compounds, we evaluated their photochromic properties in organic solvents. The UV-vis spectra of 3a,b, 9, and 10 in DCM or MeOH in the dark adapted state showed a typical maximum at about 438-444 nm, as expected for the (Z)-isomers according to previous work ((5 nm).8,11,13 Irradiation at 406 nm causes the appearance of a broad maximum of the (E)-isomers at about 447-461 nm in either DCM or MeOH (Table 3). Presumably, the data collected in Table 3 refer to general observations related to (a) differences in the substitution pattern in the 4′-position at the phenyl residue and (b) differences in the polarity of the solvents as well as (c) in the functional group polarity.8,11-13 In all cases, photoisomerization is readily observed at 406 nm (Z-to-E isomerization) and at 480 nm (E-to-Z isomerization) showing isosbestic points and reversibility during irradiation for several days. The quantitative analysis of the isomer ratios in the photostationary states (pss) at 406 and 480 nm was determined by 1H NMR spectroscopy, since, e.g., the vinyl protons of both isomers give diagnostic signals in the 1H NMR spectra (Table 3). In the dark adapted state for compound 3a (CD2Cl2) and 10 (CD3OD), the (Z)-isomer is observed exclusively, whereas for compound 9 (CD3OD), the Z:E ratio is 93:7. The thermal E-to-Z isomerization proceeds rather slowly with a half-life of 138 h for 3a in CD2Cl2 and of 20 and 22 h for 9 and 10, respectively, in CD3OD at 25 °C. For the 7-alkoxy carbonyl-substituted hemithioindigos evaluated in this study, more enriched 143

Table 3. Photochromic Properties of Hemithioindigo Compounds at Room Temperature λmax (nm) compound

solvent

Z

Ed

3a 3a 3b 9 10 10

CH2Cl2 CH3OH CH2Cl2 CH3OH CH2Cl2 CH3OH

440 438 438 444 438 442

450 457 447 461 450 450

 (dm3 M-1 cm-1) (Z)-isomer

isosbestic points

CEa,b (%)

13830 7453 10846 8667 6290 6155

376,455 379,456 365,454 481,461 366,449 365,457

84e

t1/2 (h) 138e

CZa,c (%) 95e

90e 80f

20.5f

81f

82f

22f

81f

a Ratios were determined by 1H NMR spectroscopy. b Conversion to the (E)-isomer determined in the pss (λ ) 406 nm). c Conversion to the (Z)-isomer determined in the pss (λ ) 480 nm). d Determined in the pss upon illumination with 406 nm. e CD2Cl2, 25 °C. f CD3OD, 25 °C.

samples in both isomeric states and improved thermal stabilities were determined under illumination in comparison to 4-, 5-, and 6-alkyl-substituted hemithioindigos reported previously.8,11 In conclusion, we have synthesized and characterized novel photochromic hemithioindigo-based dicarboxylic acid esters and ω-amino acid derivatives. These chromophores exhibit useful optical properties for the photocontrol of the structure and function of biomolecules. We are currently evaluating the application of 10 in solid-phase peptide synthesis of photoswitchable peptides.

144

Acknowledgment. This work was supported by the Deutsche Forschungsgemeinschaft (Sonderforschungsbereich 498). For the donation of equipment, we thank Aventis Pharma, Germany. We also thank A. G. Woolley, University of Toronto, Canada, for useful discussions. Supporting Information Available: Full experimental procedures and characterization data for 3a-c, 4, and 6-11. This material is available free of charge via the Internet at http://pubs.acs.org. OL027102+

Org. Lett., Vol. 5, No. 2, 2003